PedAM

Pediatric Disease Annotations & Medicines


	purpura fulminans

Disease ID	517
Disease	purpura fulminans
Definition	A severe, rapidly fatal reaction occurring most commonly in children following an infectious illness. It is characterized by large, rapidly spreading skin hemorrhages, fever, or shock. Purpura fulminans often accompanies or is triggered by DISSEMINATED INTRAVASCULAR COAGULATION.
Synonym	fulminans purpura fulminans, purpura purpura fulminans (disorder) purpura fulminans [disease/finding] purpura, fulminans
DOID	DOID:0060538
UMLS	C0085650
MeSH	D055665
SNOMED-CT	SNOMEDCT_US_2016_09_01:13507004
Comorbidity	UMLS \| Disease \| Sentences' Count(Total Sentences:19) C0012739 \| disseminated intravascular coagulation \| 3 C0242666 \| protein s deficiency \| 2 C0012739 \| disseminated intravascular coagulation (dic) \| 2 C0032285 \| pneumoniae \| 2 C0035078 \| renal failure \| 1 C0600327 \| toxic shock syndrome \| 1 C0152966 \| pneumococcal sepsis \| 1 C0026272 \| mixed connective tissue disease \| 1 C0008049 \| varicella infection \| 1 C0021400 \| influenzae \| 1 C0022661 \| chronic renal failure \| 1 C0025306 \| meningococcal sepsis \| 1 C0085278 \| antiphospholipid antibody syndrome \| 1 C0041471 \| typhus \| 1 C0398623 \| thrombophilia \| 1 C0003864 \| arthritis \| 1 C0024790 \| paroxysmal nocturnal haemoglobinuria \| 1 C0008049 \| varicella \| 1 C0009782 \| connective tissue disease \| 1
Curated Gene	Entrez_id \| Symbol \| Resource(Total Genes:1) PROC \| 5624 \| CTD_human
Inferring Gene	(Waiting for update.)
Text Mined Gene	Entrez_id \| Symbol \| Score \| Resource(Total Genes:34) 1361 \| CPB2 \| DISEASES 5411 \| PNN \| DISEASES 10544 \| PROCR \| DISEASES 5054 \| SERPINE1 \| DISEASES 7035 \| TFPI \| DISEASES 5624 \| PROC \| DISEASES 5199 \| CFP \| DISEASES 27130 \| INVS \| DISEASES 11043 \| MID2 \| DISEASES 671 \| BPI \| DISEASES 5286 \| PIK3C2A \| DISEASES 23082 \| PPRC1 \| DISEASES 1409 \| CRYAA \| DISEASES 2147 \| F2 \| DISEASES 5340 \| PLG \| DISEASES 9377 \| COX5A \| DISEASES 5345 \| SERPINF2 \| DISEASES 716 \| C1S \| DISEASES 2152 \| F3 \| DISEASES 5265 \| SERPINA1 \| DISEASES 462 \| SERPINC1 \| DISEASES 55788 \| LMBRD1 \| DISEASES 959 \| CD40LG \| DISEASES 29952 \| DPP7 \| DISEASES 4524 \| MTHFR \| DISEASES 7056 \| THBD \| DISEASES 2592 \| GALT \| DISEASES 114899 \| C1QTNF3 \| DISEASES 2524 \| FUT2 \| DISEASES 5627 \| PROS1 \| DISEASES 133396 \| IL31RA \| DISEASES 721 \| C4B \| DISEASES 4700 \| NDUFA6 \| DISEASES 11012 \| KLK11 \| DISEASES
Locus	(Waiting for update.)

Disease ID	517
Disease	purpura fulminans
Integrated Phenotype	(Waiting for update.)
Text Mined Phenotype	HPO \| Name \| Sentences' Count(Total Phenotypes:12) HP:0100806 \| Sepsis \| 3 HP:0005521 \| Disseminated intravascular coagulation \| 3 HP:0011880 \| Acute disseminated intravascular coagulation \| 1 HP:0001369 \| Arthritis \| 1 HP:0100724 \| Hypercoagulability \| 1 HP:0002045 \| Abnormally low body temperature \| 1 HP:0003774 \| End-stage renal failure \| 1 HP:0003613 \| Antiphospholipid antibodies \| 1 HP:0000083 \| Renal insufficiency \| 1 HP:0100758 \| Gangrene \| 1 HP:0003256 \| Coagulopathy \| 1 HP:0004818 \| Paroxysmal nocturnal hemoglobinuria \| 1

Disease ID	517
Disease	purpura fulminans
Manually Symptom	UMLS \| Name(Total Manually Symptoms:9) C2598155 \| pain C1550639 \| fistula C1521999 \| acute myocardial infarction C0584984 \| heterozygous factor v leiden mutation C0522224 \| palsy C0398625 \| protein c deficiency C0339141 \| orbital haemorrhage C0025309 \| meningoencephalitis C0025306 \| meningococcal sepsis
Text Mined Symptom	UMLS \| Name \| Sentences' Count(Total Symptoms:1) C0025306 \| meningococcal sepsis \| 1

Manually Genotype(Total Text Mining Genotypes:0)
(Waiting for update.)

All Snps(Total Genotypes:0)
(Waiting for update.)

GWASdb Annotation(Total Genotypes:0)
(Waiting for update.)

GWASdb Snp Trait(Total Genotypes:0)
(Waiting for update.)

Mapped by lexical matching(Total Items:0)
(Waiting for update.)

Mapped by homologous gene(Total Items:0)
(Waiting for update.)

Chemical(Total Drugs:3)
CUI	ChemicalName	ChemicalID	CasRN	DiseaseName	DiseaseID	DirectEvidence	PubMedIDs
C0085650	acetaminophen	D000082	103-90-2	purpura fulminans	MESH:D055665	marker/mechanism	8215490
C0085650	diclofenac	D004008	15307-86-5	purpura fulminans	MESH:D055665	marker/mechanism	12219272
C0085650	phenytoin	D010672	57-41-0	purpura fulminans	MESH:D055665	marker/mechanism	1147459

FDA approved drug and dosage information(Total Drugs:4)
DiseaseID	Drug_name	active_ingredients	strength	Dosage Form/Route	Marketing Status	TE code	RLD	RS
MESH:D055665	ofirmev	acetaminophen	1GM/100ML (10MG/ML)	SOLUTION;IV (INFUSION)	Prescription	AP	Yes	Yes
MESH:D055665	ofirmev	acetaminophen	1GM/100ML (10MG/ML)	SOLUTION;IV (INFUSION)	Prescription	AP	Yes	Yes
MESH:D055665	acetaminophen	acetaminophen	650MG	SUPPOSITORY;RECTAL	Over-the-counter	None	Yes	Yes
MESH:D055665	acetaminophen	acetaminophen	650MG	SUPPOSITORY;RECTAL	Over-the-counter	None	Yes	Yes

FDA labeling changes(Total Drugs:4)
DiseaseID	Pediatric_Labeling_Date	Trade_Name	Generic_Name_or_Proper_Name	Indications Studied	Label Changes Summary	Product Labeling	BPCA(B)	PREA(P)	BPCA(B) and PREA(P)	Pediatric Rule (R)	Sponsor	Pediatric Exclusivity Granted Date	NNPS
MESH:D055665	2/11/2010	ofirmev	acetaminophen	Management of mild-to-moderate pain, for the management of moderate-to-severe pain with adjunctive opioid analgesics, and for the reduction of fever	The safety and effectiveness of Ofirmev for the treatment of acute pain and fever in pediatric patients ages 2 years and older is supported by evidence from adequate and well-controlled studies of Ofirmev in adults. Additional safety and PK data was collected in 355 from premature neonates to adolescents. The effectiveness of Ofirmev for the treatment of acute pain and fever has not been studied in pediatric patients < 2 years of age.The PK exposure of Ofirmev observed in children and adolescents is similar to adults, but higher in neonates and infants. Dosing simulations from PK data in infants and neonates suggest that dose reductions of 33% in infants 1 month to < 2 years of age, and 50% in neonates up to 28 days, with a minimum dosing interval of 6 hours, will produce a PK exposure similar to that observed in children age 2 years and olderMost common adverse reactions in pediatric patients were nausea, vomiting, constipation, pruritus, agitation, and atelectasis.Information on dosing, clinical studies, adverse reactions and PK parametersNew dosage form and route of administration	Labeling	-	P	-	-	Cadence	-	FALSE'
MESH:D055665	01/27/2017	ofirmev	acetaminophen	Treatmeny of pain and fever in pediatric patients birth to 2 years	Treatment of pain Efficacy was not demonstrated in pediatric patients younger than 2 years in a double-blind, placebo-controlled study of 198 pediatric patients younger than 2 years. Pediatric patients less than 2 years of age, including neonates from 28 to 40 weeks gestational age at birth, were randomized to receive opioid plus acetaminophen or opioid plus placebo. No difference in analgesic effect of intravenous acetaminophen, measured by assessment of reduced need for additional opioid treatment for pain control, was observed. Treatment of fever The safety and effectiveness for the treatment of fever in pediatric patients, including premature neonates born at 32 weeks or greater gestation is supported by adequate and well-controlled studies of Ofirmev in adults, clinical studies in 244 pediatric patients 2 years and older, and safety and pharmacokinetic data from 239 patients younger than 2 years including neonates 32 weeks or greater gestational age. Information on dosing, clinical trials. Postmarketing study.	Labeling	-	-	B,P	-	Mallinckrodt	11/7/2016	FALSE
MESH:D055665	2/11/2010	ofirmev	acetaminophen	Management of mild-to-moderate pain, for the management of moderate-to-severe pain with adjunctive opioid analgesics, and for the reduction of fever	The safety and effectiveness of Ofirmev for the treatment of acute pain and fever in pediatric patients ages 2 years and older is supported by evidence from adequate and well-controlled studies of Ofirmev in adults. Additional safety and PK data was collected in 355 from premature neonates to adolescents. The effectiveness of Ofirmev for the treatment of acute pain and fever has not been studied in pediatric patients < 2 years of age.The PK exposure of Ofirmev observed in children and adolescents is similar to adults, but higher in neonates and infants. Dosing simulations from PK data in infants and neonates suggest that dose reductions of 33% in infants 1 month to < 2 years of age, and 50% in neonates up to 28 days, with a minimum dosing interval of 6 hours, will produce a PK exposure similar to that observed in children age 2 years and olderMost common adverse reactions in pediatric patients were nausea, vomiting, constipation, pruritus, agitation, and atelectasis.Information on dosing, clinical studies, adverse reactions and PK parametersNew dosage form and route of administration	Labeling	-	P	-	-	Cadence	-	FALSE'
MESH:D055665	01/27/2017	ofirmev	acetaminophen	Treatmeny of pain and fever in pediatric patients birth to 2 years	Treatment of pain Efficacy was not demonstrated in pediatric patients younger than 2 years in a double-blind, placebo-controlled study of 198 pediatric patients younger than 2 years. Pediatric patients less than 2 years of age, including neonates from 28 to 40 weeks gestational age at birth, were randomized to receive opioid plus acetaminophen or opioid plus placebo. No difference in analgesic effect of intravenous acetaminophen, measured by assessment of reduced need for additional opioid treatment for pain control, was observed. Treatment of fever The safety and effectiveness for the treatment of fever in pediatric patients, including premature neonates born at 32 weeks or greater gestation is supported by adequate and well-controlled studies of Ofirmev in adults, clinical studies in 244 pediatric patients 2 years and older, and safety and pharmacokinetic data from 239 patients younger than 2 years including neonates 32 weeks or greater gestational age. Information on dosing, clinical trials. Postmarketing study.	Labeling	-	-	B,P	-	Mallinckrodt	11/7/2016	FALSE

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